(Fenneropenaeus chinensis)

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1 ( ) (Fenneropenaeus chinensis) MCP-KP 3 C 16.38e -2.58t 0.32e -0.1t C 18.7e -2.57t 0.26e -0.12t C 15.08e 1.49t +0.65e -0.09t 15.74e 10.38t (t (1/2)α ) 0.269, h (t (1/2)β ) 6.921, h (V β ) 1.287, L/kg (C s ) 0.129, L/(h kg) (A u,c ) 0.755, L/(h kg) (F) 90.20% 97.58% (Fenneropenaeus chinensis) (HPLC) S948 A florfenicol Schering-Plough D [1] [2~6] [7~10] [11] [12] [13] [14] (Fenneropenaeus chinensis) BA906A (1981- ) lijian@ysfri.ac.cn 64

2 A.R HPLC HPLC A.R Agilent1100 (HPLC) HPLC 223 nm - 27/ ml/min 20 µl g 19~22 2/ g 100 mg/l mg/l 100 mg/l mg kg 15 mg/kg mg 20 g 15 g ,0.25,0.5,1,2,4,7,11,16,24 h 0.5,1,2,4,7,11,16,24 h 8 1 ml ml 2.0 ml 2 ml 30s r/min 20 min 10mL ml 1 min 0.45 µm HPLC g 0.1,1,10 mg/l 3 2 h 3 1 d d MCP-KP mg/l y=50.937x, r= mg/l ,1,10 mg/l % 83.89% 87.23% 6.40% 1.66% 0.42% 8.15% 1.40% 4.35% Marine Sciences/Vol.30,No.7/

3 mg/kg C 16.38e -2.58t 0.32e -0.1t C 18.7e -2.57t 0.26e -0.12t C 15.08e 1.49t +0.65e -0.09t 15.74e 10.38t min mg/kg F F A u,c /A u,c D /D 1 Fig.1 Plasma concentration-time profile of florfenicol in 3 Fenneropenaeus chinensis following a single intravenous, intramuscular and oral administration mg/kg 5 min 5 min 15 min 30 min 30 min 2 h 2 h 3 1 mg/ L 1 Tab.1 Pharmacokinetic parameters of florfenicol in Fennerope naeus chinensis following a single intravenous, intramuscular and oral administration D (mg/kg) C 0 (mg/l) A (mg/l) B (mg/l) α (h -1 ) β (h -1 ) K a (h -1 ) K 12 (h -1 ) K 21 (h -1 ) K el (h -1 ) t (1/2)Ka (h) T (1/2)α (h) t (1/2)β (h) A u,c ((h mg)/l) T max (h) C max (ng/l) V β (L/kg) C s (L/(h kg)) F (%) D C 0 A,B α,β K a K 12 K 21 K el t (1/2)Ka t (1/2)α, t (1/2)β A u,c T max C max V β C s F 3 α 3 β V β V β 66

4 V β 1 V β 1 C s A u,c [12] [2] 78.5 [3] 81 [4] [5] 96.6 [6] [11] 96.5 [7] [11] 3.2 [7] [14] Bernt [7] 12.2 h [15] h h mg/kg C max T max 1 Bernt 10 mg/kg C max 4.0 mg/l T max 10.3 h [7] [11] 20 mg/kg C max T max 7.45 mg/l 2 h [12] 20 mg/kg C max T max 7.45 mg/l 2 h α 0.22 h -1 [7] [14] [11] 0.086, L/(h kg) Bretzlaff -OH -F [1],,. [J].Animal Science Abroad, 1999, 26(3): [2] Atef M, EL-GENDI A Y, Amer A M M, et al. Pharmacokinetics properties of florfenicol in Egyptian goats [J]. Deutsche Tierortliche Wochenschrift, 2000,107(4): [3] Lobell R D, Varma F J, Johnson J C, et al. Pharmacokinetics of florfenicol following intravenous and intramuscular doses to cattle [J]. Journal of Pharmacology Therapeutics, 1994,17: [4] Mckelllller Q A,Varma K J. Pharmacokinetics and tolerance of florfenicol in Equidae [J]. Equine Vet J, 1996,28(3): [5] El Banna H A. Pharmacokinetics of florfenicol in normal and Pasteurella-infected Muscovy ducks [J]. British Poultry Science, 1998,39: [6] Afifi N A, EI-Sooud K A. Tissue concentration and pharmacokinetics of florfenicol in broiler chickens [J]. British Poultry Science, 1997, 38(4): Marine Sciences/Vol.30,No.7/

5 [7] Bernt M, Tor E H, Kanval J V, et al. Single dose pharmacokinetic study of florfenicol in Atlantic salmon (Salmo salar) in seawater at 11 [J]. Aquaculture,1993, 112:1 11. [8] Ole B S, Øivind B. Efficacy of orally administered florfenicol and oxolinic acid for the treatment of vibriosis in cod (Gadus morhua) [J]. Aquaculture, 2004,235: [9] Lund n T, Miettinen S, Lonnstrom L -G, et al. Effect of florfenicol on the immune response of rainbow trout (Oncorhynchus mykiss) [J]. Veterinary and Immunopathology, 1999,67: [10] Chue V, Larry J S, Guy R S, et al. Liquid chromatographic determination of florfenicol in the plasma of multiple species of fish [J]. Journal of Chormatogrphy B, 2002,780: [11]. [J] [12]. [J]., [13]. [J] [14]. [J] [15],,,. [J].,2003,27(1): Single dose pharmacokinetics of florfenicol in Fenneropenaeus chinensis LI Jing-yun 1,2, LI Jian 1, WANG Qun 1, ZHAN Wen-bin 2 Yellow Sea Fisheries Research Institute, Chinese Academy of Fishery Science, Qingdao ,China; 2. Fishery College, Ocean University of China, Qingdao ,China) Received Oct.,18,2004 Key words: florfenicol Fenneropenaeus chinensis pharmacokinetics; high performance liquid chromatography HPLC Abstract: The pharmacokinetics of intravenously, intramuscularly and orally administered florfenicol were determined in Fenneropenaeus chinensis.the study was performed at 19~22.A dose of 15mg/ kg body mass was administered either intravenously or intramuscularly. The oral dose was13.56 mg/kg body mass. At 8~10 time points, from h to 24 h after administration, blood was sampled from 8 individual shrimps in each group. The plasma was assayed for florfenicol using an HPLC method. The pharmacokinetic modling of the results was performed using the computer program MCP-KP. Following the three administrations, the plasma concentration time data of florfenicol were all best described by two-compartment open model. The important parameters of intravenous, intramuscular and oral administrations were listed. The volumes of distribution( V β )were 1.287,1.293,2.421 L/kg, the total body clearance(c s )was 0.129,0.138,0.213 L/(h kg), the elimination halflives ( t (1/2)β ) were 5.91,7.57,8.01 h, the peak plasma concentrations(c max ) were 6.970,6.396,2.772 mg/l,and were estimated to occur at 0.206,0.239,0.605 h (T max ) following dosing. The bioavailabilities (F) of intramuscular and oral administrations were 90.20% and 97.58%. 68

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